| Literature DB >> 19167332 |
Yuxia Zhang1, Libo Yan, Zhi Zhou, Peiguo Yang, E Tian, Kai Zhang, Yu Zhao, Zhipeng Li, Bing Song, Jinghua Han, Long Miao, Hong Zhang.
Abstract
How autophagy, an evolutionarily conserved intracellular catabolic system for bulk degradation, selectively degrades protein aggregates is poorly understood. Here, we show that several maternally derived germ P granule components are selectively eliminated by autophagy in somatic cells during C. elegans embryogenesis. The activity of sepa-1 is required for the degradation of these P granule components and for their accumulation into aggregates, termed PGL granules, in autophagy mutants. SEPA-1 forms protein aggregates and is also a preferential target of autophagy. SEPA-1 directly binds to the P granule component PGL-3 and also to the autophagy protein LGG-1/Atg8. SEPA-1 aggregates consistently colocalize with PGL granules and with LGG-1 puncta. Thus, SEPA-1 functions as a bridging molecule in mediating the specific recognition and degradation of P granule components by autophagy. Our study reveals a mechanism for preferential degradation of protein aggregates by autophagy and emphasizes the physiological significance of selective autophagy during animal development.Entities:
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Year: 2009 PMID: 19167332 DOI: 10.1016/j.cell.2008.12.022
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582